Session Information
Session Type: ACR Concurrent Abstract Session
Session Time: 9:00AM-10:30AM
Background/Purpose: Glucocorticoids (GC) are associated with substantial treatment morbidity. New immunomodulatory agents offer the possibility of limiting GC exposure. To assess the comparative benefits of such agents, investigators must accurately measure their ability to prevent or reverse GC-related toxicity. No comprehensive instrument for measuring GC toxicity has previously been developed. We aimed to develop a GC Toxicity Index (GTI) to assess GC-related morbidity and GC-sparing ability of new agents.
Methods: Nineteen experts from 11 subspecialties participated. Ten experts were from the United States; 9 from Canada, Europe, or Australia. Group consensus methods and multi-criteria decision analysis were utilized. The development process included ten 1-hour conference calls, group work between calls and a 12-hour face-to-face meeting. GTI components The GTI is composed of the Composite GTI (CGTI) and the Specific List. The CGTI reflects GC toxicity that is likely to change over the course of a clinical trial. The toxicities included in the CGTI occur commonly, vary with GC exposure, and are weighted and scored. The Specific List is designed to capture GC toxicity not included in the CGTI. The CGTI was evaluated by application to paper cases by the investigators and an external group of 17 subspecialists.
Results: Item inclusion and definitions Thirty-one toxicity items derived from the literature were included in the CGTI, and 23 were included in the Specific List (Table). Definitions were developed by experts using group consensus methods. The CGTI items reflect both improvement and worsening of GC toxicity and account for medication effects (e.g., anti-hypertensives) in scoring. The 31 mutually-exclusive CGTI items are organized in order of severity within nine domains. Only one item in each domain can be scored. Weighting and evaluation of the CGTI Relative weights for each item in the CGTI were derived at a face-to-face meeting utilizing multi-criteria decision analysis. CGTI evaluation showed high inter-rater agreement (investigators kappa 0.88, external raters kappa 0.90). To assess the degree to which the CGTI corresponds to expert clinical judgment, participants ranked 15 cases by clinical judgment in order of highest to lowest GC toxicity. Expert rankings were then compared to case ranking by the CGTI, yielding excellent agreement (investigators weighted kappa 0.87, external raters weighted kappa 0.77).
Conclusion: We describe the development and initial evaluation of the GTI – a comprehensive instrument intended primarily for use in prospective, randomized clinical trials for the assessment of GC toxicity. The GTI can be used across clinical disciplines in trials that employ GCs to assess the comparative value of GC-sparing therapies, and to measure the impact of GC toxicity. Table – Composite GTI and Specific List
| Composite GTI |
Item Weight |
Specific List | |
| Body mass index |
|
||
| Improvement in BMI |
-8 |
Major increase in BMI | |
| No change in BMI |
0 |
||
| Moderate increase in BMI |
21 |
||
| Major increase in BMI |
36 |
||
| Glucose tolerance |
|
||
| Improvement in glucose tolerance |
-8 |
Diabetic retinopathy | |
| No change in glucose tolerance |
0 |
Diabetic nephropathy | |
| Worsening of glucose tolerance |
32 |
Diabetic neuropathy | |
| Worsening of glucose tolerance despite treatment |
44 |
||
| Blood pressure |
|
||
| Improvement in blood pressure |
-10 |
Hypertensive emergency | |
| No change in blood pressure |
0 |
Posterior reversible encephalopathy syndrome | |
| Worsening hypertension |
19 |
||
| Worsening hypertension despite treatment |
44 |
||
| Lipids |
|
||
| Improvement in lipids |
-9 |
||
| No change in lipids |
0 |
||
| Worsening hyperlipidemia |
10 |
||
| Worsening hyperlipidemia despite treatment |
30 |
||
| Bone density |
|
||
| Improvement in bone density |
-1 |
Major decrease in bone density | |
| No change in bone density |
0 |
Insufficiency fracture | |
| Decrease in bone density |
29 |
||
| Steroid myopathy |
|
||
| No steroid myopathy |
0 |
Severe steroid myopathy | |
| Mild steroid myopathy |
9 |
||
| Moderate steroid myopathy or greater |
63 |
||
| Skin toxicity |
|
||
| No skin toxicity |
0 |
Severe skin toxicity | |
| Mild skin toxicity |
8 |
||
| Moderate skin toxicity or greater |
26 |
||
| Neuropsychiatric toxicity |
|
||
| No neuropsychiatric symptoms |
0 |
Psychosis | |
| Mild neuropsychiatric symptoms |
11 |
GG-induced violence | |
| Moderate neuropsychiatric symptoms or greater |
74 |
Other severe neuropsychiatric symptoms | |
| Infection |
|
||
| No significant infection |
0 |
Grade 4 infection | |
| Oral/vaginal candidiasis or uncomplicated zoster |
19 |
Grade 5 infection | |
| Grade 3 infection or greater |
93 |
||
| Endocrine |
|
Adrenal insufficiency | |
| Gastrointestinal |
|
Perforation | |
|
|
Peptic ulcer disease | ||
| Musculoskeletal |
|
Avascular necrosis | |
|
|
Tendon rupture | ||
| Ocular |
|
Central serous retinopathy | |
|
|
Intraocular pressure elevation | ||
|
|
Posterior subcapsular cataract | ||
| Total |
-36 to 439 |
||
To cite this abstract in AMA style:
Miloslavsky E, Naden RP, Bijlsma JW, Brogan P, Brown S, Brunetta P, Buttgereit F, Choi HK, Dicaire JF, Gelfand J, Heaney L, Lightstone L, Lu L, Murrell D, Petri M, Rosenbaum JT, Saag K, Urowitz M, Winthrop KL, Stone JH. Development of a Glucocorticoid Toxicity Index Using Multi-Criteria Decision Analysis [abstract]. Arthritis Rheumatol. 2016; 68 (suppl 10). https://acrabstracts.org/abstract/development-of-a-glucocorticoid-toxicity-index-using-multi-criteria-decision-analysis/. Accessed .« Back to 2016 ACR/ARHP Annual Meeting
ACR Meeting Abstracts - https://acrabstracts.org/abstract/development-of-a-glucocorticoid-toxicity-index-using-multi-criteria-decision-analysis/